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NCT05726825 Clinical Trial

Efficacy of add-on Plasma Exchange as an Adjunctive Strategy Against Septic Shock

Septic Shock Clinical Trial

EXCHANGE-2

Official title:
Randomized, Prospective, Multicenter, Open-label, Controlled, Parallel-group Trial Investigating the Efficacy of add-on Plasma Exchange as an Adjunctive Strategy Against Septic Shock - 2

Clinical Trial Details — Status: Not yet recruiting

Administrative data
NCT number NCT05726825
Other study ID # EXCHANGE-2
Secondary ID
Status Not yet recruiting
Phase N/A
First received
Last updated
Start date November 28, 2023
Est. completion date January 31, 2027

Study information
Verified date September 2023
Source Hannover Medical School
Contact Sascha David, Prof. Dr.
Phone +41 44 255 8653
Email sascha.david@usz.ch
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

Randomized, prospective, multicenter, open-label, controlled, parallel-group interventional trial to test the adjunctive effect of therapeutic plasma exchange in patients with early septic shock.

Description:

Sepsis is defined as a life-threatening organ dysfunction caused by a dysregulated host response to an infection; in septic shock profound circulatory, cellular and metabolic abnormalities are associated with an even higher mortality. Sepsis is a major healthcare problem, affecting millions of individuals around the world each year. Its incidence appears to be rising, and the mortality caused by septic shock in Germany in 2015 remains extraordinarily high (58.8%). It is well known - from the pathophysiological point of view - that these patients do not die from their infection per se but rather from multiple organ failure caused by their own overwhelming host response. This fact is so fundamental that it has been implemented as a key part of the 2016 sepsis definition (SEPSIS-3). Despite tremendous efforts during the last decades, innovative approaches targeting this fundamental hallmark of the disease, thereby reducing organ dysfunction, are lacking. Undoubtedly, there is an unmet need to expand the current standard of care for these patients by a more specific intervention. The investigators hypothesize that early Therapeutic Plasma Exchange (TPE) in the most severely ill individuals will dampen the injurious maladaptive host response by removing injurious mediators thereby limiting organ dysfunction. The potential impact of this trial is of immense clinical relevance as it evaluates a promising adjunctive treatment option for a patient cohort suffering from an extraordinary high mortality. A positive trial result could truly change the current standard of care (SOC) - that is mostly supportive - of septic shock patients. Of note, there is neither a patent nor a direct commercial interest in such a trial.

Recruitment information / eligibility
Status Not yet recruiting
Enrollment 274
Est. completion date January 31, 2027
Est. primary completion date August 31, 2026
Accepts healthy volunteers No
Gender All
Age group 18 Years to 80 Years
Eligibility Inclusion Criteria: - New onset of septic shock (< 24 hrs), (SEPSIS-3 definition) - Norepinephrine (NE) dose = 0.4 µg/kg/min = 30 min OR NE = 0.3 µg/kg/min + vasopressin (any dose) - Established vascular access suitable for plasma exchange independent of study inclusion (due to established indication of RRT, expected need for RRT within the next 48 hours or other medical reasons as assessed by treating physician team) Exclusion Criteria: - Age < 18 or > 80 years - Urogenital focus of infection - Pregnancy - Heparin-induced thrombocytopenia - Known reaction against fresh frozen plasma (FFP)

Study Design

Related Conditions & MeSH terms

Intervention

Device:
Therapeutic Plasma Exchange (TPE)
The TPE treatment will be initiated within 6 hrs after randomization. Duration of TPE treatment is approximately 120-180 minutes. An additional second TPE can be performed if the patient remains vasopressor dependent = 0.4 ug/kg/min after 24 hours following the first TPE procedure. Both unfractionated heparin (UFH) and citrate may be used as anticoagulant medication. To ensure treatment comparability between different patients, we will replace plasma in a fixed ratio of 1.2 x the individual patient's total plasma fluid.

Locations
Country Name City State
Austria University Hospital Innsbruck Innsbruck
Austria University Hospital Vienna Vienna
Germany St. Joseph Hospital Berlin
Germany University Hospital Berlin Charite Berlin
Germany University Hospital Bonn Bonn
Germany Hospital Braunschweig Braunschweig
Germany Hospital Bremerhaven Bremerhaven
Germany Hospital Cologne Meerheim Cologne
Germany University Hospital Cologne Cologne
Germany University Hospital Erlangen Erlangen
Germany University Hospital Essen Essen
Germany University Hospital Halle Halle
Germany University Hospital Hamburg (UKE) Hamburg
Germany Hannover Medical School Anesthesiology Hannover
Germany Hannover Medical School Internal Medicine Hannover
Germany University Hospital Heidelberg Heidelberg
Germany University Hospital Jena Jena
Germany University Hospital Kiel Kiel
Germany Hospital Magdeburg Magdeburg
Germany University Hospital Muenster Anesthesiology Muenster
Germany University Hospital Munich (TUM) Anesthesiology Munich
Germany University Hospital Munich (TUM) Internal Medicine Munich
Germany University Hospital Rostock Rostock
Switzerland University Hospital Bern Bern
Switzerland University Hospital Zurich Zurich

Sponsors (1)
Lead Sponsor Collaborator
Hannover Medical School

Countries where clinical trial is conducted

Austria,  Germany,  Switzerland, 

References & Publications (6)

David S, Bode C, Putensen C, Welte T, Stahl K; EXCHANGE study group. Adjuvant therapeutic plasma exchange in septic shock. Intensive Care Med. 2021 Mar;47(3):352-354. doi: 10.1007/s00134-020-06339-1. Epub 2021 Jan 20. No abstract available. — View Citation

Knaup H, Stahl K, Schmidt BMW, Idowu TO, Busch M, Wiesner O, Welte T, Haller H, Kielstein JT, Hoeper MM, David S. Early therapeutic plasma exchange in septic shock: a prospective open-label nonrandomized pilot study focusing on safety, hemodynamics, vascular barrier function, and biologic markers. Crit Care. 2018 Oct 30;22(1):285. doi: 10.1186/s13054-018-2220-9. — View Citation

Stahl K, Bikker R, Seeliger B, Schmidt JJ, Schenk H, Schmidt BMW, Welte T, Haller H, Hoeper MM, Brand K, David S. Effect of Therapeutic Plasma Exchange on Immunoglobulin Deficiency in Early and Severe Septic Shock. J Intensive Care Med. 2021 Dec;36(12):1491-1497. doi: 10.1177/0885066620965169. Epub 2020 Oct 16. — View Citation

Stahl K, Hillebrand UC, Kiyan Y, Seeliger B, Schmidt JJ, Schenk H, Pape T, Schmidt BMW, Welte T, Hoeper MM, Sauer A, Wygrecka M, Bode C, Wedemeyer H, Haller H, David S. Effects of therapeutic plasma exchange on the endothelial glycocalyx in septic shock. Intensive Care Med Exp. 2021 Nov 24;9(1):57. doi: 10.1186/s40635-021-00417-4. — View Citation

Stahl K, Schmidt JJ, Seeliger B, Schmidt BMW, Welte T, Haller H, Hoeper MM, Budde U, Bode C, David S. Effect of therapeutic plasma exchange on endothelial activation and coagulation-related parameters in septic shock. Crit Care. 2020 Mar 2;24(1):71. doi: 10.1186/s13054-020-2799-5. — View Citation

Stahl K, Wand P, Seeliger B, Wendel-Garcia PD, Schmidt JJ, Schmidt BMW, Sauer A, Lehmann F, Budde U, Busch M, Wiesner O, Welte T, Haller H, Wedemeyer H, Putensen C, Hoeper MM, Bode C, David S. Clinical and biochemical endpoints and predictors of response to plasma exchange in septic shock: results from a randomized controlled trial. Crit Care. 2022 May 12;26(1):134. doi: 10.1186/s13054-022-04003-2. — View Citation

Outcome
Type Measure Description Time frame Safety issue
Other Safety Endpoints includes: Incidence of bleeding, allergic reactions, Transfusion associated lung injury (TRALI), severe thrombocytopenia (< 5000/µl) and (other) severe adverse events (SAEs) from randomization until day 7 following randomization
Primary 28-day mortality from randomization up to 28 days following randomization
Secondary Mean daily Sequential Organ Failure Score (SOFA) score over the first 7 days (KEY secondary outcome) Per-patient mean daily SOFA score over the first 7 days, ranging from 0-24 points with higher scores indicating more severe organ dysfunction from randomization up to 7 days following randomization
Secondary Organ support free days until day 28 (KEY secondary outcome) total days free of invasive ventilation, vasopressors/inotrops and renal replacement therapy (RRT) until day 28 from randomization up to 28 days following randomization
Secondary 90-day mortality from randomization up to 90 days following randomization
Secondary Intensive Care unit (ICU) length of stay total days in ICU from randomization until ICU discharge
Secondary Hospital length of stay total days in hospital from randomization until hospital discharge
Secondary Basic Hemodynamics includes: Norepinephrine- [µg/kg/min], Dobutamine [µg/kg/min], Epinephrine- [µg/kg/min] and Vasopressin-dose [U/kg/min], Vasocative-inotropic (VIS) Score with higher scores indicating higher vasopressor/inotropic support, Mean arterial pressure (MAP, [mmHg]), Heart Rate (HR, [1/min]), Central venous pressure (CVP, [mmHg]) and Central-Venous Oxygen Saturation (ScvO2, [%]) at 0 and 12 hrs, d1-7 at days 1-7 following randomization
Secondary Extended Hemodynamics includes: Cardiac Index (CI, [l/min/m2]), Global End-Diastolic Volume Index (GEDI, [ml/m2]), Sytemic Vascular Resistance Index (SVRI, [dyn*s*cm-5*m2]), Stroke Volume Variation (SVV, [%] ), Extravascular Lung Water Index (ELWI, [ml/kg]) and Pulmonar Vascular Permeability Index (PVPI) at at 0 and 12 hrs, d1-7 at days 1-7 following randomization
Secondary Arterial blood gas analysis includes: pH, PCO2 [mmHg], HCO3- [mmol], PO2 [mmHg], Lactate [mmol/l] at 0 and 12 hrs, d1-7 at days 1-7 following randomization
Secondary Respiratory function includes: pO2/FiO2, Tidal Volume (VT, [ml]), Positive End-Exspiratory Pressure (PEEP, [cmH2O]), Peak-Pressure (Ppeak, [cmH2O]), Plateau-Pressure (Pplat, [cmH2O]), Respiratory Rate (RR, [1/min]), Inspiratory Time (Tinsp, [s]), Inspiratory-Flow and End-tidal-CO2 (etCO2, [mmHg]) at 0 and 12 hrs, d1-7 at days 1-7 following randomization
Secondary Renal function includes: Presence of Acute kindey injury (AKI), AKI stage (KDIGO definition) stage 1-3 with higher stage indicating worse renal function, Need for Renal Replacement Therapy (RRT), Estimated Glomerular Filtration Rate (eGFR following CKD-EPI equation) [ml/min], Fluid intake [ml/d], Urine output [ml/d], Ultrafiltration and Net daily fluid balance [ml/d] at 0 and 12 hrs, d1-7 and at ICU discharge at days 1-7 following randomization and at ICU discharge
Secondary Liver Function includes: Bilirubin, Aspartate aminotransferase (AST, [U/l]), Alanine aminotransferase (ALT, [U/l]), Alkaline phosphatase (AP, [U/l]), Gamma-glutamyl transferase (GGT, [U/l]), Cholinesterase (CHE, [kU/l]) and Albumin [g/l] at 0 and 12 hrs, d1-7 and at ICU discharge at days 1-7 following randomization and at ICU discharge
Secondary Sepsis associated coagulopathy includes: Differential blood count including schistocytes [%], Fibrinogen [g/l] , D-Dimer [mg/l], International Normalized Ratio (INR), Lactate dehydrogenase (LDH, [U/l]), Antithrombin-III (AT-III, [%]), Protein C [%] and International Society on Thrombosis and Hemostasis- Disseminated Intravscular Coagulation Score (ISTH-DIC, [U/l]) ranging from 0-8 points with higher values indication more severe DIC at 0 and 12 hrs, d1-7, A disintegrin and metalloproteinase with a thrombospondin type 1 motif, member 13 (ADAMTS13, [%]) and von-Willebrand-Factor Antigen (vWF:Ag,[IU/l]) at 0 and 24 hrs at days 1-7 following randomization
Secondary Inflammatory response includes: C-reactive protein (CRP, [mg/l]), Procalcitonin (PCT, [ug/l]), Interleukin-6 (IL-6, [ng/ml]), Ferritin [ug/l] and Neutrophil/Lymphocyte ratio at 0 and 12 hrs, d1-7 at days 1-7 following randomization
Secondary Cardiac function includes: Creatine kinase (CK, [U/l]), Myoglobin [ug/l], Troponin T [ng/l], NT-proBNP [ng/l] at 0 and 12 hrs, d1-7 and at ICU discharge at days 1-7 following randomization and at ICU discharge
Secondary Secondary infections includes: incidence and type of secondary infections until ICU and hospital discharge, incidence of viral (HSV, EBV, CMV) reactivation at d7 and d14 from randomization until hospital discharge
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